| Literature DB >> 29424951 |
Thomas J Cummins1, Noemi Kedei2, Agnes Czikora2, Nancy E Lewin2, Sharon Kirk1, Mark E Petersen1, Kevin M McGowan1, Jin-Qiu Chen3, Xiaoling Luo3, Randall C Johnson4, Sarangan Ravichandran4, Peter M Blumberg2, Gary E Keck1.
Abstract
To investigate the cellular distribution of tumor-promoting vs. non-tumor-promoting bryostatin analogues, we synthesized fluorescently labeled variants of two bryostatin derivatives that have previously shown either phorbol ester-like or bryostatin-like biological activity in U937 leukemia cells. These new fluorescent analogues both displayed high affinity for protein kinase C (PKC) binding and retained the basic properties of the parent unlabeled compounds in U937 assays. The fluorescent compounds showed similar patterns of intracellular distribution in cells, however; this argues against an existing hypothesis that various patterns of intracellular distribution are responsible for differences in biological activity. Upon further characterization, the fluorescent compounds revealed a slow rate of cellular uptake; correspondingly, they showed reduced activity for cellular responses that were only transient upon treatment with phorbol ester or bryostatin 1.Entities:
Keywords: Merle; bryostatin; fluorescent probes; protein kinase C; pyran annulation
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Year: 2018 PMID: 29424951 PMCID: PMC6980389 DOI: 10.1002/cbic.201700655
Source DB: PubMed Journal: Chembiochem ISSN: 1439-4227 Impact factor: 3.164